Inducing the “re-development state” of periodontal ligament cells via tuning macrophage mediated immune microenvironment

[Display omitted] •Proposing the “developmental engineering” strategy in promoting cementum-PDL-alveolar bone complex formation in periodontium regeneration.•Discovering that tuning macrophage immune response can be effective to perform this developmental engineering strategy mediated by PDLCs.•Consideration of applying periodontal development engineering strategy in periodontal multi-tissue regeneration was shown. Periodontal regeneration, specifically the restoration of the cementum-periodontal ligament (PDL)-alveolar bone complex, remains a formidable challenge in the field of regenerative dentistry. In light of periodontal development, harnessing the multi-tissue developmental capabilities of periodontal ligament cells (PDLCs) and reinitiating the periodontal developmental process hold great promise as an effective strategy to foster the regeneration of the periodontal complex. This study aims to delve into the potential effects of the macrophage-mediated immune microenvironment on the “developmental engineering” regeneration strategy and its underlying molecular mechanisms. In this study, we conducted a comprehensive examination of the periodontium developmental process in the rat mandibular first molar using histological staining. Through the induction of diverse immune microenvironments in macrophages, we evaluated their potential effects on periodontal re-development events using a cytokine array. Additionally, we investigated PDLC-mediated periodontal re-development events under these distinct immune microenvironments through transcriptome sequencing and relevant functional assays. Furthermore, the underlying molecular mechanism was also performed. The activation of development-related functions in PDLCs proved challenging due to their declined activity. However, our findings suggest that modulating the macrophage immune response can effectively regulate PDLCs-mediated periodontium development-related events. The M1 type macrophage immune microenvironment was found to promote PDLC activities associated with epithelial-mesenchymal transition, fiber degradation, osteoclastogenesis, and inflammation through the Wnt, IL-17, and TNF signaling pathways. Conversely, the M2 type macrophage immune microenvironment demonstrated superiority in inducing epithelium induction, fibers formation, and mineralization performance of PDLCs by upregulating the TGFβ and PI3K-Akt signaling pathway. The results of this study could provide some favorable theoretical bases